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      Effects of bone marrow on the microenvironment of the human pancreatic islet: A Protein Profile Approach.

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          Abstract

          Stem cells are a new therapeutic modality that may support the viability and function of human organs and tissue. Our previous studies have revealed that human allogeneic bone marrow (BM) sustains pancreatic β cell function and survival. This paper examines whether BM creates a microenvironment that supports human pancreatic islets in vitro by evaluating 107 proteins in culture media from BM, islet, and islet/bone marrow (IB) with mass spectrometry. Proteins were considered up- or down-regulated if p-values < 0.05 and fold change was greater than 2 fold I VS. IB. In addition, proteins identified that were uniquely found in islets co-cultured with bone marrow, but not in islets or bone marrow. A 95% protein probability was used as a threshold. Twenty three proteins were upregulated, and sixteen proteins were downregulated. The function of each protein is listed based on the protein database, which include structural proteins (9 upregulated, 4 downregulated); anti-protease and anti-endopeptidase enzymes (8 upregulated); cation binding proteins (6 up-regulated). Six proteins were uniquely identified in islet co-cultured with bone marrow. Three are anti-proteases or anti-endopeptidases, and 1 is a structural protein. These findings suggest that BM, by changing culture media proteins, may be one of mechanisms to maintain human islet function and survival.

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          Author and article information

          Journal
          Mol. Cell. Endocrinol.
          Molecular and cellular endocrinology
          Elsevier BV
          1872-8057
          0303-7207
          Jul 15 2017
          : 450
          Affiliations
          [1 ] The Center of Stem Cell Biology, Department of Medicine, Roger Williams Hospital, Boston University, School of Medicine, Providence, RI 02908, USA.
          [2 ] The Center of Stem Cell Biology, Department of Medicine, Roger Williams Hospital, Boston University, School of Medicine, Providence, RI 02908, USA; Insure Health, Inc, 30 Quaker Lane Suite 35, Warwick, RI 02886, USA.
          [3 ] The Center of Stem Cell Biology, Department of Medicine, Roger Williams Hospital, Boston University, School of Medicine, Providence, RI 02908, USA. Electronic address: Lluo@Chartercare.org.
          Article
          S0303-7207(17)30236-8
          10.1016/j.mce.2017.04.014
          28428043
          251da7e3-213a-4402-89b7-04ea141bfa77
          History

          Bone marrow,Diabetes mellitus,Glucose stimulated insulin secretion,Human pancreatic islets,Protein mass spectrometry,STRING

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